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含α-OH-PdG.dA 碱基对的双链 DNA 的 NMR 结构:丙烯醛的诱变中间体。

NMR structure of duplex DNA containing the alpha-OH-PdG.dA base pair: a mutagenic intermediate of acrolein.

机构信息

Department of Pharmacological Sciences, Stony Brook University, School of Medicine Stony Brook, NY 11794-8651, USA.

出版信息

Biopolymers. 2010 Apr;93(4):391-401. doi: 10.1002/bip.21366.

Abstract

Acrolein, a cell metabolic product and main component of cigarette smoke, reacts with DNA generating alpha-OH-PdG lesions, which have the ability to pair with dATP during replication thereby causing G to T transversions. We describe the solution structure of an 11-mer DNA duplex containing the mutagenic alpha-OH-PdG.dA base pair intermediate, as determined by solution nuclear magnetic resonance (NMR) spectroscopy and retrained molecular dynamics (MD) simulations. The NMR data support a mostly regular right-handed helix that is only perturbed at its center by the presence of the lesion. Undamaged residues of the duplex are in anti orientation, forming standard Watson-Crick base pairs alignments. Duplication of proton signals at and near the damaged base pair reveals the presence of two enantiomeric duplexes, thus establishing the exocyclic nature of the lesion. The alpha-OH-PdG adduct assumes a syn conformation pairing to its partner dA base that is protonated at pH 6.6. The three-dimensional structure obtained by restrained molecular dynamics simulations show hydrogen bond interactions that stabilize alpha-OH-PdG in a syn conformation and across the lesion containing base pair. We discuss the implications of the structures for the mutagenic bypass of acrolein lesions.

摘要

丙烯醛是一种细胞代谢产物和香烟烟雾的主要成分,它与 DNA 反应生成α-OH-PdG 损伤,这种损伤在复制过程中能够与 dATP 配对,从而导致 G 突变为 T。我们描述了一种含有诱变α-OH-PdG.dA 碱基对中间体的 11 -mer DNA 双链体的溶液结构,这是通过溶液核磁共振(NMR)光谱和重新训练的分子动力学(MD)模拟确定的。NMR 数据支持一个主要为右手螺旋的结构,仅在其中心受到损伤的存在的干扰。双链体未受损的残基呈反式取向,形成标准的 Watson-Crick 碱基对排列。在受损碱基对附近和附近的质子信号的复制揭示了两种对映体双链体的存在,从而确定了损伤的外消旋性质。α-OH-PdG 加合物采用与在 pH 6.6 下质子化的其伙伴 dA 碱基配对的顺式构象。通过受约束的分子动力学模拟获得的三维结构显示了稳定α-OH-PdG 处于顺式构象和穿过含有损伤碱基对的氢键相互作用。我们讨论了这些结构对丙烯醛损伤的突变体旁路的意义。

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本文引用的文献

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Nucleic Acids Res. 2009 Apr;37(7):2153-63. doi: 10.1093/nar/gkp076. Epub 2009 Feb 17.
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